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The Transcriptional Corepressor NAB2 Inhibits NGF-induced Differentiation of PC12 Cells

机译:转录corepressor NAB2抑制NGF诱导的PC12细胞分化。

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摘要

The PC12 pheochromocytoma cell line responds to NGF by undergoing growth arrest and proceeding to differentiate toward a neuronal phenotype. Among the early genetic events triggered by NGF in PC12 cells are the rapid activation of the zinc finger transcription factor Egr1/NGFI-A, and a slightly delayed induction of NAB2, a corepressor that inhibits Egr1 transcriptional activity. We found that stably transfected PC12 cells expressing high levels of NAB2 do not differentiate, but rather continue to proliferate in response to NGF. Inhibition of PC12 differentiation by NAB2 overexpression was confirmed using two additional experimental approaches, transient transfection, and adenoviral infection. Early events in the NGF signaling cascade, such as activation of MAP kinase and induction of immediate-early genes, were unaltered in the NAB2-overexpressing PC12 cell lines. However, induction of delayed NGF response genes such as TGF-β1 and MMP-3 was inhibited. Furthermore, NAB2 overexpression led to downregulation of p21WAF1, a molecule previously shown to play a pivotal role in the ability of PC12 cells to undergo growth arrest and commit to differentiation in response to NGF. Cotransfection with p21WAF1 restored the ability of NAB2-overexpressing PC12 cells to differentiate in response to NGF.
机译:PC12嗜铬细胞瘤细胞系通过生长停滞并向神经元表型分化而对NGF作出反应。 NGF在PC12细胞中触发的早期遗传事件包括锌指转录因子Egr1 / NGFI-A的快速激活,以及NAB2的诱导稍有延迟,NAB2是抑制Egr1转录活性的核心抑制剂。我们发现表达高水平NAB2的稳定转染的PC12细胞没有分化,而是响应NGF而继续增殖。使用另外两种实验方法,瞬时转染和腺病毒感染,证实了NAB2过表达抑制PC12分化。在过表达NAB2的PC12细胞系中,NGF信号级联反应的早期事件,如MAP激酶的激活和即早基因的诱导,没有改变。但是,抑制了延迟的NGF应答基因如TGF-β1和MMP-3的诱导。此外,NAB2的过表达导致p21 WAF1 的下调,p21 WAF1 是一种先前显示在PC12细胞经历生长停滞并响应NGF分化的能力中起关键作用的分子。与p21 WAF1 的共转染恢复了过表达NAB2的PC12细胞分化为NGF的能力。

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